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系统评价:用于溃疡性结肠炎治疗的口服美沙拉嗪制剂和美沙拉嗪前体药物的药代动力学特征

Systematic review: the pharmacokinetic profiles of oral mesalazine formulations and mesalazine pro-drugs used in the management of ulcerative colitis.

作者信息

Sandborn W J, Hanauer S B

机构信息

Division of Gastroenterology and Hepatology, Mayo Clinic, 200 First Street SW, Rochester, MN 55905, USA.

出版信息

Aliment Pharmacol Ther. 2003 Jan;17(1):29-42. doi: 10.1046/j.1365-2036.2003.01408.x.

DOI:10.1046/j.1365-2036.2003.01408.x
PMID:12492730
Abstract

AIM

: To quantify through systematic review the pharmacokinetic profiles of the oral delayed release and sustained release mesalazine (5-aminosalicylate, 5ASA) formulations (Asacol, Salofalk, Mesasal, Claversal, Pentasa) and pro-drugs (sulfasalazine, olsalazine, balsalazide) used in the management of ulcerative colitis.

METHODS

: Selected articles had: (1) adult healthy volunteers or patients with ulcerative colitis and (2) quantification of pharmacokinetic data to include, at a minimum, urinary excretion of total 5ASA [5ASA plus N-Acetyl-5ASA (N-Ac-5ASA)].

DATA COLLECTION AND ANALYSIS

: Pharmacokinetic data (Tmax, Cmax, AUC, urinary excretion, faecal excretion) of 5ASA, its major metabolite N-Acetyl-5ASA, total 5ASA, and the parent pro-drug compounds was extracted.

MAIN RESULTS

: The summary results for urinary excretion of total 5ASA over 24-96 h in all subjects (either mean or median) were: sulfasalazine mean 11-33% or median 22%; olsalazine mean 14-31% or median 16-27%; balsalazide mean 12-35% or median 20%; Asacol mean 10-35% or median 18-40%; Pentasa mean 15-53% or median 23-34%; Salofalk, Mesasal and Claversal mean 27-56% or median 31-44%. The summary results for faecal excretion of total 5ASA over 24-96 h in all subjects (either mean or median) were: sulfasalazine mean 23-75% or median 38%; olsalazine mean 47-50% or median 17-36%; balsalazide mean 46% or median 22%; Asacol mean 40-64% or median 20-56%; Pentasa mean 12-51% or median 39-59%; Salofalk, Mesasal and Claversal mean 37-44% or median 23-35%.

CONCLUSIONS

: The systemic exposure to 5ASA, as measured by urinary excretion of total 5ASA, and the faecal excretion of total 5ASA is comparable for all oral mesalazine formulations and pro-drugs. Thus, selection of a mesalazine therapy for the treatment of ulcerative colitis should be based on other factors such as efficacy, dose-response, toxicity of the parent compound and its metabolites, compliance issues related to dose forms and dosing schedules, and costs.

摘要

目的

通过系统评价量化用于溃疡性结肠炎治疗的口服缓释和控释美沙拉嗪(5-氨基水杨酸,5ASA)制剂(艾迪莎、颇得斯安、美沙拉嗪、克拉莎尔、潘太欣)及前体药物(柳氮磺胺吡啶、奥沙拉嗪、巴柳氮)的药代动力学特征。

方法

入选的文章需满足:(1)成年健康志愿者或溃疡性结肠炎患者;(2)药代动力学数据的量化,至少包括总5ASA(5ASA加N-乙酰-5ASA(N-Ac-5ASA))的尿排泄量。

数据收集与分析

提取5ASA、其主要代谢物N-乙酰-5ASA、总5ASA及母体前体药物化合物的药代动力学数据(达峰时间、峰浓度、曲线下面积、尿排泄量、粪便排泄量)。

主要结果

所有受试者在24 - 96小时内总5ASA尿排泄量的汇总结果(均值或中位数)为:柳氮磺胺吡啶均值11 - 33%或中位数22%;奥沙拉嗪均值14 - 31%或中位数16 - 27%;巴柳氮均值12 - 35%或中位数20%;艾迪莎均值10 - 35%或中位数18 - 40%;潘太欣均值15 - 53%或中位数23 - 34%;颇得斯安、美沙拉嗪和克拉莎尔均值27 - 56%或中位数31 - 44%。所有受试者在24 - 96小时内总5ASA粪便排泄量的汇总结果(均值或中位数)为:柳氮磺胺吡啶均值23 - 75%或中位数38%;奥沙拉嗪均值47 - 50%或中位数17 - 36%;巴柳氮均值46%或中位数22%;艾迪莎均值40 - 64%或中位数20 - 56%;潘太欣均值12 - 51%或中位数39 - 59%;颇得斯安、美沙拉嗪和克拉莎尔均值37 - 44%或中位数23 - 35%。

结论

通过总5ASA的尿排泄量及总5ASA的粪便排泄量衡量,所有口服美沙拉嗪制剂及前体药物对5ASA的全身暴露量相当。因此,选择美沙拉嗪疗法治疗溃疡性结肠炎应基于其他因素,如疗效、剂量反应、母体化合物及其代谢物的毒性、与剂型和给药方案相关的依从性问题以及成本。

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